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Reversion to methionine independence by malignant rat and SV40-transformed human fibroblasts.
Authors:R M Hoffman  S J Jacobsen  R W Erbe
Institution:1. Genetics Unit, Children''s Service, Massachusetts General Hospital Harvard Medical School, Boston, MA 02114 USA;2. Center for Human Genetics Harvard Medical School, Boston, MA 02114 USA;3. Department of Pediatrics Harvard Medical School, Boston, MA 02114 USA
Abstract:Although many lines of malignant and transformed cells are unable to grow in folate- and cobalamin-supplemented medium in which methionine is replaced by homocysteine its immediate metabolic precursor, rare cells from these lines regained the normal ability to grow under these conditions. Six revertant lines, one from Walker-256 rat breast carcinoma cells and five from SV40-transformed human fibroblasts, have been characterized with regard to growth and three measures of methionine biosynthetic capacity: methionine synthetase and methylenetetrahydrofolate reductase activities in cell extracts, and uptake of label from 5-14C]methyltetrahydrofolate by intact cells. When all three measures of methionine biosynthetic capacity were considered, two revertants isolated from SV40-transformed cells had regained the ability to grow like normal cells in homocysteine medium without substantial changes in these measures. Increased methionine biosynthesis thus is not a prerequisite to reversion of the methionine auxotrophy present in the transformed parental lines.
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